Suppr超能文献

接触敏感性转移中的抑制机制。对Ly2抑制性细胞活性所需的I-J+分子的分析。

Mechanisms of suppression in the transfer of contact sensitivity. Analysis of an I-J+ molecule required for Ly2 suppressor cell activity.

作者信息

Ptak W, Gershon R K, Flood P M

出版信息

J Exp Med. 1983 Dec 1;158(6):1822-35. doi: 10.1084/jem.158.6.1822.

Abstract

The passive transfer of contact sensitivity (CS) by immune cells can be inhibited with an antigen-specific T suppressor factor. This factor is composed of two subfactors: an antigen-specific subfactor made by an Ly1+ cell (PC1-F) and a antigen nonspecific subfactor made by an Ly2+ T cell (TNBSA-F). The suppressive activity of the complete factor can be eliminated by depleting the assay population of Ly2+ cells, even though it is the Ly1+ cell in the population that transfers the adoptive immunity. This suggests that the Ly2+ cell in the assay population is needed to transduce the suppressive signal to the Ly1+ effector cell of DTH. We found that an Ly2+ cell from immune animals could be induced to produce a cell free subfactor that overcame the requirement for this Ttrans cell in the suppression of CS by TsF. The induction required only PC1-F, TNP-coupled spleen cells, and resulted in the production of an antigen-nonspecific I-J+ subfactor by immune Ly2+, I-J+ cells. The need for the Ly2+ transducer cell could also be overcome by addition of an I-J+ molecule secreted by Ly1 T cells hyperimmunized to SRBC. A suppressor complex made from mixing the I-J+ molecule with TNBSA-F could directly suppress the functional activity of immune T cells not only to transfer CS, but also to deliver help to B cells in an in vitro PFC response. This suppressive complex is antigen-nonspecific and does not require Ly2+ T cells in the assay population for suppressive activity. These results indicate that effector factors of the suppressor circuit require two molecules; one that contains the functional suppressor material and one that serves as a "schlepper," a molecule needed to deliver the suppression to the appropriate target cell. The ability to construct a functional suppressor complex from two subfactors raised against different antigens, using different immunization procedures, which were isolated from factors exhibiting different functional activities suggests that certain cells of the immune system may play a universal role in "transducing" the suppressive signal.

摘要

免疫细胞对接触敏感性(CS)的被动转移可被一种抗原特异性T抑制因子所抑制。该因子由两个亚因子组成:一个由Ly1⁺细胞产生的抗原特异性亚因子(PC1 - F)和一个由Ly2⁺T细胞产生的抗原非特异性亚因子(TNBSA - F)。即使群体中负责传递过继免疫的是Ly1⁺细胞,但通过耗尽Ly2⁺细胞的检测群体,完整因子的抑制活性仍可被消除。这表明检测群体中的Ly2⁺细胞是将抑制信号传递给迟发型超敏反应(DTH)的Ly1⁺效应细胞所必需的。我们发现,来自免疫动物的Ly2⁺细胞可被诱导产生一种无细胞亚因子,该亚因子在TsF抑制CS的过程中可取代对这种Ttrans细胞的需求。这种诱导仅需要PC1 - F、TNP偶联的脾细胞,并导致免疫的Ly2⁺、I - J⁺细胞产生一种抗原非特异性的I - J⁺亚因子。通过添加由对SRBC高度免疫的Ly1 T细胞分泌的I - J⁺分子,也可克服对Ly2⁺转导细胞的需求。由I - J⁺分子与TNBSA - F混合制成的抑制复合物不仅可直接抑制免疫T细胞传递CS的功能活性,还可在体外PFC反应中为B细胞提供辅助。这种抑制复合物是抗原非特异性的,且在检测群体中发挥抑制活性时不需要Ly2⁺T细胞。这些结果表明,抑制回路的效应因子需要两种分子;一种包含功能性抑制物质,另一种作为“转运分子”,即一种将抑制作用传递给合适靶细胞所需的分子。利用不同的免疫程序从表现出不同功能活性的因子中分离出针对不同抗原的两个亚因子,构建出功能性抑制复合物的能力表明,免疫系统的某些细胞可能在“转导”抑制信号方面发挥普遍作用。

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